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新生儿免疫挑战改变雌性大鼠的生殖发育。

Neonatal immune challenge alters reproductive development in the female rat.

机构信息

Laboratory of Neuroimmunology, School of Psychology, Faculty of Science and IT, The University of Newcastle, Australia.

出版信息

Horm Behav. 2012 Aug;62(3):345-55. doi: 10.1016/j.yhbeh.2012.02.005. Epub 2012 Feb 14.

Abstract

Neonatal lipopolysaccharide (LPS) exposure alters neuroendocrine, immune and behavioural responses in adult rats. Recent findings indicate that neonatal LPS treatment may have a more pronounced effect on the mating behaviours of females compared to males. The current study further explored the impact of neonatal inflammation on reproductive development in the female rat. Wistar rats were administered LPS (0.05 mg/kg, i.p.) or saline (equivolume) on postnatal days (PNDs) 3 and 5. The immediate effect of treatment was assessed on plasma corticosterone and tyrosine hydroxylase (TH) phosphorylation in the adrenal medulla. Weight gain and vaginal opening were recorded, and oestrous cyclicity was monitored post-puberty and in late adulthood. Blood and ovaries were collected throughout development to assess HPA and HPG hormones and to examine ovarian morphology. Reproductive success in the first (F1) generation and reproductive development in the second (F2) generation were also assessed. Neonatal LPS exposure resulted in increased TH phosphorylation in the neonatal adrenals. LPS treatment increased the corticosterone concentrations of females as juveniles, adolescents and adults, and reduced FSH in adolescence. Increased catch-up growth was evident in LPS-treated females, prompting earlier onset of puberty. Diminished follicular reserve was observed in neonatally LPS-treated females along with the advanced reproductive senescence. While fertility rates were not compromised, higher mortality and morbidity were observed in litters born to LPS-treated mothers. Female offspring of LPS-treated mothers displayed increased corticosterone on PND 14, increased catch-up growth and delayed emergence of the first oestrous cycle. No differences in any of the parameters assessed were observed in F2 males. These data suggest that neonatal immunological challenge has a profound impact on the female reproductive development, via the alteration of metabolic and neuroendocrine factors which regulate sexual maturation. Evidence of altered development in the female, but not male offspring of LPS-treated dams suggests increased susceptibility of females to the deleterious effects of neonatal immunological stress and its possible transferability to a subsequent generation.

摘要

新生大鼠脂多糖(LPS)暴露会改变其神经内分泌、免疫和行为反应。最近的研究结果表明,与雄性相比,新生 LPS 处理可能对雌性的交配行为产生更显著的影响。本研究进一步探讨了新生期炎症对雌性大鼠生殖发育的影响。Wistar 大鼠于生后第 3 天和第 5 天(PND)腹腔内注射 LPS(0.05mg/kg)或生理盐水(等容量)。治疗的即时影响通过检测肾上腺髓质中的皮质酮和酪氨酸羟化酶(TH)磷酸化来评估。记录体重增加和阴道开口,并在青春期后和成年晚期监测发情周期。在整个发育过程中收集血液和卵巢,以评估 HPA 和 HPG 激素并检查卵巢形态。还评估了第一代(F1)的生殖成功率和第二代(F2)的生殖发育。新生 LPS 暴露导致新生肾上腺中 TH 磷酸化增加。LPS 处理增加了雌性青少年、青少年和成年期的皮质酮浓度,并降低了青春期的 FSH。LPS 处理的雌性出现追赶性生长,青春期提前开始。与生殖衰老提前相关,还观察到新生 LPS 处理的雌性卵泡储备减少。尽管生育率没有受到损害,但 LPS 处理母亲所生的后代死亡率和发病率更高。LPS 处理母亲的雌性后代在 PND14 时表现出更高的皮质酮、追赶性生长和首次发情周期的延迟出现。在 F2 雄性中未观察到任何评估参数的差异。这些数据表明,新生免疫挑战通过改变调节性成熟的代谢和神经内分泌因素,对雌性生殖发育产生深远影响。LPS 处理母鼠的雌性后代而非雄性后代出现发育改变,表明雌性对新生免疫应激的有害影响更为敏感,并且这种影响可能传递给下一代。

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